Haemodynamic effects of a new dihydropyridine calcium entry blocker, S‐12968‐(−), in a rat model of cardiovascular calcium overload

1 The haemodynamic effects of S-12968-(−), a new dihydropyridine calcium entry blocker (enantiomer of S-11568), were compared with those of the stereoisomer, S-12967-(+), nifedipine, and sodium nitroprusside. 2 A first experiment was performed in conscious, young male rats chronically implanted with femoral artery and vein cannula and repeated in rats previously treated with vitamin D3 and nicotine. Such treatment produces marked vascular calcium overload, especially of the compliance arteries, with no overt sign of toxicity as far as can be judged from the plasma profile. 3 In conscious rats the hypotensive effects of S-12968-(−), nifedipine and sodium nitroprusside were of similar potency. The falls in blood pressure produced by nifedipine and sodium nitroprusside were accompanied by reflex tachycardia which was less marked in the vascular calcium overload model. S-12968-(−) did not induce reflex tachycardia. S-12967-(+) increased blood pressure in both models. 4 A second experiment was performed in open-chest pentobarbitone-anaesthetized rats with electromagnetic flowprobes on the ascending aorta. In controls the falls in blood pressure produced by low doses (0.1 and 0.3 mg kg−1, i.v.) of S-12968-(−) were accompanied by falls in total peripheral resistance. The higher dose (1 mg kg−1, i.v.) of S-12968-(−) produced no change in total peripheral resistance, and in rats pretreated with vitamin D3 and nicotine, cardiac output fell. 5 In conclusion, S-12968-(−) appears to have a dual action and to lower blood pressure at higher doses at least in part by a cardiac effect. This phenomenon is more pronounced in rats pretreated with vitamin D3 and nicotine. 6 S-12967-(+) resembles a calcium channel activator in this model.